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Electromyography (EMG), Electroencephalography (EEG), and Neurophysiology in Clinical Practice
Monday, February 23, 2015 Ritz-Carlton Amelia Island, Florida
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CME Activity Description
This course is designed as a review of techniques and topics pertaining to Clinical Neurophysiology which includes: basic physiology; pathophysiology; EEG; evoked potentials; EMG; movement disorders; and intraoperative monitoring. There is a focus on clinical correlation of various neurophysiological tests used for the evaluation of patients with epilepsy, sleep disorders, movement disorders, peripheral nerve, and neuromuscular disorders. Presentations will be made by members of the staff of Mayo Clinic and faculty of the Mayo Clinic College of Medicine from the Department of Neurology in Jacksonville, Florida; Rochester, Minnesota; and Scottsdale, Arizona. CME Activity Objectives
Upon conclusion of this program, participants should be able to: • Develop a logical approach to the use of standard clinical electrophysiological techniques in
the evaluation of common and uncommon neuromuscular disorders • Identify technical pitfalls associated with NCS and needle EMG and understand methods to
correct and minimize technical problems • Interpret the findings and clinical significance of abnormalities on nerve conduction studies • Recognize and interpret the significance of EMG waveforms on needle EMG • Identify technical pitfalls associated with EEG and the normal and variant patterns of
pediatric and adult patients • Interpret the findings and clinical significance of abnormalities on EEG studies • Integrate the various clinical neurophysiology studies (evoked potentials, autonomic
tests, sleep studies, vestibular testing) in the evaluation of patients with disorders of the central nervous system
Attendance at this Mayo Clinic activity does not indicate nor guarantee competence or proficiency in the performance of any procedures which may be discussed or taught in this activity. Intended Audience
This course is intended for neurologists and physiatrists interested in the basics of clinical EMG, EEG, and Neurophysiology. Attendance at this Mayo course does not indicate nor guarantee competence or proficiency in the performance of any procedures that may be discussed or taught in this course. Continuing Education Credit
College of Medicine, Mayo Clinic, is accredited by the Accreditation Council for Continuing Medical Education to provide continuing medical education for physicians. College of Medicine, Mayo Clinic, designates this live activity for a maximum of 55.5 AMA PRA Category 1 Credits™ and Self-Assessment 8.0 AMA PRA Category 1 Credits™. Physicians should claim only the credit commensurate with the extent of their participation in the activity. American Board of Psychiatry and Neurology Mayo Clinic College of Medicine is accredited by the Accreditation Council for Continuing Medical Education to provide continuing medical education for physicians. Mayo Clinic College of Medicine designates this Self-Assessment for up to 8.0 AMA PRA Category 1 Credits™. Physicians should claim only the credit commensurate with the extent of their participation in the activity.
The American Board of Psychiatry and Neurology has reviewed the "EMG, EEG and Clinical Neurophysiology, Feb 22-28, 2015 course, (awarding Self-Assessment 8.0 AMA PRA Category 1 Credits™) and has approved this program as part of a comprehensive self-assessment program, which is mandated by the ABMS as a necessary component of Maintenance of Certification. CME Record of Attendance
A Record of Attendance is provided to you during on-site registration. The Record of Attendance allows attendees to calculate their own credits of participation in the educational activity. The total number of credits participants can earn per day is noted on the Record of Attendance. Below each day is a line to record the actual number of credits during which you participated in the educational activity. It is recommended that you record your actual credits daily as you proceed through the CME activity. Upon conclusion of the CME activity, please total the number of credits you have recorded on the top half of the form, sign it, and return it with your evaluation to the registration desk. The bottom half of the form represents your Record of Attendance, which you must retain for your records. Please make sure the number of credits claimed in both sections coincide. No other documentation is provided to you after this CME activity. The Record of Attendance has replaced the certificate. The Record of Attendance can be used for requesting credits in accordance with state licensing boards, specialty societies, or other professional associations. CME Activity Evaluation
The overall CME activity evaluation will be emailed following the activity to the email address that was provided when you registered. The CME activity evaluation is brief and will only take a few minutes to complete. Faculty evaluation forms were offered to a sampling of the registrants. Completed faculty evaluation forms should be returned to the registration desk at the conclusion of the CME activity. If you wish to participate in evaluating the faculty, please stop at the registration desk to inquire if extra evaluation forms are available. Your feedback is very important to us and will be used for planning future programs, as well as identifying faculty strengths and opportunity for growth. Syllabus and Internet Access
A link to the syllabus will be provided to all attendees. Participants are invited to bring their laptops to the meeting room(s). Due to copyright issues or revisions, some slides may be shown during a presentation, but not provided within the syllabus.
Recording Device Policy
No recording devices, audio or visual, may be used during Mayo Clinic College of Medicine CPD activities. Duplication, distribution, or excerpting of this program, without the express written permission of Mayo Clinic, is strictly prohibited. All of the proceedings of this program, including the presentation of scientific papers, are intended for limited publication only, and all property rights in the material presented, including common-law copyright, are expressly reserved by the Faculty and/or Mayo Clinic. No statement of presentation made is to be regarded as dedicated to the public domain. Any sound reproduction, transcript or other use of the material presented at this CME activity without the permission of Mayo Clinic is prohibited to the full extent of common-law copyright in such material. Electronic Devices
Please turn all electronic devices (cellular telephones, pagers, etc.) to silent mode. As a courtesy to the presenters and other participants, phone calls should be taken outside of the general session.
Faculty Course Director(s) Devon I. Rubin, M.D. and Jerry J. Shih, M.D.
Guest
Randa G. Jarrar, M.D. Child Neurology Phoenix Children’s Hospital Phoenix, Arizona
Mayo Clinic
Jeffrey W. Britton, M.D. Professor of Neurology Department of Neurology
Katherine H. Noe, M.D., Ph.D. Associate Professor of Neurology Department of Neurology
Jonathan L. Carter, M.D. Associate Professor of Neurology Department of Neurology
Eric T. Payne, M.D. Associate Professor of Neurology Department of Neurology
Gregory D. Cascino, M.D. Professor of Neurology Department of Neurology
Mark A. Ross, M.D. Professor of Neurology Department of Neurology
Brian A. Crum, M.D. Associate Professor of Neurology Department of Neurology
Devon I. Rubin, M.D. Professor of Neurology Department of Neurology
Elliot L. Dimberg, M.D. Assistant Professor of Neurology Department of Neurology
Raj D. Sheth, M.D. Professor of Neurology Department of Neurology
Joseph F. Drazkowski, M.D. Professor of Neurology Department of Neurology
Jerry J. Shih, M.D. Associate Professor of Neurology Department of Neurology
P. James Dyck, M.D. Professor of Neurology Department of Neurology
Michael H. Silber, M.B., Ch.B. Assistant Professor of Neurology Department of Neurology
Brent P. Goodman, M.D. Assistant Professor of Neurology Department of Neurology
Wolfgang Singer, M.D. Associate Professor of Neurology Department of Neurology
Lyell K. Jones, Jr., M.D. Assistant Professor of Neurology Department of Neurology
Elson So, M.D. Professor of Neurology Department of Neurology
Kathleen D. Kennelly, M.D., Ph.D. Assistant Professor of Neurology Department of Neurology
Eric J. Sorenson, M.D. Professor of Neurology Department of Neurology
Terrence D. Lagerlund, M.D., Ph.D. Associate Professor of Neurology Department of Neurology
Jeffrey A. Strommen, M.D. Assistant Professor of Neurology Department of Neurology
Ruple S. Laughlin, M.D. Assistant Professor of Neurology Department of Neurology
William Tatum, D.O. Professor of Neurology Department of Neurology
Michelle L. Mauermann, M.D. Assistant Professor of Neurology Department of Neurology
James C. Watson, M.D. Assistant Professor of Neurology Department of Neurology
Katherine C. Nickels, M.D. Assistant Professor of Neurology Department of Neurology
Gregory A. Worrell, M.D., Ph.D. Professor of Neurology Department of Neurology
David A. Zapala, Ph.D. Associate Professor of Audiology Department of Audiology
Faculty, Planning Committee and Provider Disclosure Summary
Electromyography (EMG), Electroencephalography (EEG), and Neurophysiology in Clinical Practice February 22 – 28, 2015 Ritz-Carlton Amelia Island, Florida
As a provider accredited by ACCME, Mayo Clinic College of Medicine (Mayo School of CPD) must ensure balance, independence, objectivity and scientific rigor in its educational activities. Course Director(s), Planning Committee Members, Faculty, and all others who are in a position to control the content of this educational activity are required to disclose all relevant financial relationships with any commercial interest related to the subject matter of the educational activity. Safeguards against commercial bias have been put in place. Faculty also will disclose any off label and/or investigational use of pharmaceuticals or instruments discussed in their presentation. Disclosure of these relevant financial relationships will be published in activity materials so those participants in the activity may formulate their own judgments regarding the presentation.
Listed below are individuals with control of the content of this program who have disclosed… Relevant financial relationship(s) with industry:
Name Nature of Relationship Company Katherine H. Noe, M.D. Grant/Research Support NeuroPace, Inc. Gregory A. Worrell, M.D., Ph.D.
Grant/Research Support Stock Shareholder (self-managed)
NIH NeuroOne, Inc.
No relevant financial relationship(s) with industry:
Name Jeffrey W. Britton, M.D. Katherine C. Nickels, M.D. Jonathan L. Carter, M.D. Eric T. Payne, M.D. Gregory D. Cascino, M.D. Mark A. Ross, M.D. Brian A. Crum, M.D. Devon I. Rubin, M.D. Elliot L. Dimberg, M.D. Jerry J. Shih, M.D. Joseph F. Drazkowski, M.D. Michael H. Silber, M.B Ch.B. P. James Dyck, M.D. Wolfgang Singer, M.D. Randa G. Jarrar, M.D. Benn E. Smith, M.D. Lyell Jones, M.D. Elson L. So, M.D. Kathleen D. Kennelly, M.D., Ph.D. Eric J. Sorenson, M.D. Terrance D. Lagerlund, M.D., Ph.D. William O. Tatum, D.O. Ruple S. Laughlin, M.D. David A. Zapala, Ph.D. Michelle L. Mauermann, M.D.
References to off-label and/or investigational usage(s) of pharmaceuticals or instruments in their presentation:
Name Manufacturer/Provider Product/Device None
Commercial Support
Electromyography (EMG),
Electroencephalography (EEG), and Neurophysiology in Clinical Practice
February 22 – 28, 2015 This activity is supported in part by educational and in-kind grants from the
following companies in accordance with ACCME Standards: (at time of printing)
Appropriate acknowledgment will be provided at the
CME Activity
. Grants
Allergan
Eisai Grifols
Lundbeck
In-Kind
Natus
Exhibitors
Electromyography (EMG), Electroencephalography (EEG), and Neurophysiology in Clinical Practice
February 22 – 28, 2015
Cadwell Laboratories Natus
NuFactor Sunovion
Walgreens
Technique of Needle Examination(and a little golf, too)
Devon I. Rubin, M.D.Mayo Clinic
Jacksonville, FL
Objective
• Practical points to consider in the performance of needle EMG
• Methods to improve technique
• Remind of special considerations or issues to reduce risk
DEVON RUBIN’S
FIVESTEPSThe Modern Fundamentals of EMG Technique
1) Planning the Study• Clinical evaluation• Muscle selection• Special precautions
2) Performing the needle examination• Preparing the patient• Needle insertion and movement• Pain control
3) Ensuring patient relaxation & tolerance
4) Analysis of spontaneous activity5) Analysis of MUP
Case72 year-old woman with right back and leg pain referred by a neurologist for an EMG. Per MDs note: “Patient has predominantly pain in back and knee. Normal strength and reflexes on exam.”
The patient is afraid of needles and will only allow you to examine one muscle. Which would you choose?
a. Iliopsoasb. Vastus medialisc. Anterior tibialisd. Medial gastrocnemiuse. I don’t know
Step 1: Planning the StudyConsiderations
• Note distribution of weak muscles and sensory deficits
• Focal, multifocal, diffuse? • Symmetric or asymmetric?
• Note possible technical concerns• Infection precautions, Anticoagulation, Skin
abnormalities
Perform your own focused neuromuscular history and examination IN EVERY PATIENT !
Step 1: Planning the StudyConsiderations in Selection of Muscles
• Examine muscles clearly involved (weak)• Define pathophysiology (myopathic vs
neurogenic)• Ideally mild-moderately weak muscles
• Examine muscles NOT likely to be involved• Narrows localization
• Suspected myopathy: Limit to one side
Step 2: Performing the Needle Examination
• Preparing the Patient
• Needle Insertion and Movement
• Minimizing patient discomfort
• Technical problems
Needle Insertion and Movement• Muscle in “neutral”
relaxed position
• Pull skin taut & distal
• “Quick stick”
Needle MovementSmoothly in short steps (0.5 to 1 mm)
Pause 1-2 seconds to listen for slow fibs
• 3-4 passes (different angles)• 5-30 steps through muscle
Needle Movement
Methods to Improve Relaxation
• Passive limb movement
• Contraction of antagonist
• Distraction• Exceptions:
•Tongue, diaphragm, (thoracic PSP)•Spasticity, rigidity, tremor
Minimizing EMG PainPatient Preparation
• Thoroughly explain test • Reassure regarding discomfort • Warn about more painful muscles• Distract with conversation• Analgesic or mild sedatives
beforehand
Monopolar vs Concentric NeedleMonopolar Concentric
Cost Less More
Baseline stability Less More
MUP amplitude / duration
Slightly higher Slightly lower
Recording surface Larger Smaller
Pickup area Larger (multidirectional) Smaller (directional)
MUP amplitude and duration
Longer /higher Shorter / lower
Recorded noise More Less
Patient discomfort ??? (Less) ???? (More)
Monopolar vs Concentric ElectrodePain Comparison
• Pain with needle examination (n=48)
• 50-mm concentric vs 50-mm monopolar
• Small (0.5-1 mm) vs Larger steps (0.5-1 cm)
Strommen JA, Daube JR. Determinants of pain in needle electromyography. Clin Neurophysiology 112: 1414-1418, 2001.
Results: Immediate Pain
• Concentric needle• small steps significantly less painful (p < 0.001) than
larger steps• Monopolar needle
• no difference in pain with step size
• Large steps: monopolar less painful, 0.01• Small steps: no difference in needles
Minimizing EMG PainNeedle Handling Techniques
• Needle movements less than one mm.
• Brief insertional bursts
• Straight line movements with pauses• Smooth, steady movements (no jabs)• Constant muscle contraction level• Continuous discussion and feedback
Endplate Activity
• Painful, move away quickly (Turn preamplifier
on immediately after needle insertion)
• Small needle movements - more control
Spike
Noise
Detecting Hematoma by MRI following EMG
Paraspinals
n=175Caress, 1996
n=542
Paraspinal Mapping
(no warfarin)London, 2012
10
n=431
(138 aspirin)(10 warfarin)Gertken, 2011
Risk with Anticoagulation
• US following EMG, mean 30 min following needle exam
• Hematoma found in:• 2/101 pts on warfarin• 1/57 pts on aspirin or
clopidogrel • 0/51 pts in control group
• All small, subclinical
Lynch S, Boon A. Muscle Nerve 2008
In other “high risk” muscles . . .
• Majority with 50 mm needle, INR 1.6 – 4.0• 2 pts with SUBCLINICAL hematomas on US
• Tibialis posterior (9 x 1 mm) (ASA/clopidogrel)• FPL (16 x 3 mm) (warfarin, INR 2.3)
Boon AJ et al. Muscle Nerve 2012
Anticoagulation
• No defined “practice parameter” regarding “safe” level of anticoagulation
• Decision is individual• Most MDs will perform with INR < 3.0 • Thrombocytopenia less than 30,000
Technique in Anticoagulated Patients
• Limit number of muscles• Limited needle movement• Avoid deep and higher risk muscles
• Anterior compartment of leg (stay superficial)• Muscles neighboring arteries (FPL, Iliopsoas)• Paraspinals
• Prolonged, firm pressure
Lymphedema
• Risk of persistent leaking of serous fluid• Possible risk of infection• AANEM Position statement (2005):
• “reasonable caution should be exercised in performing needle examinations in lymphedematous regions.”
Cutaneous Issues
Peri-pleural Muscles• Trapezius• Cervical paraspinals• Rhomboid• Serratus anterior• Intercostal &
diaphragm• Methods:
• Slow, smooth needle movements
• Listen for short rise time MUPs
• Withdraw when rise time slows
• Listen for respiratory pattern of firing
Summary
• Remember each step of needle EMG
• Plan the study appropriately
• Minimize discomfort using SMALL needle movements
• Adjust technique in special circumstances
• Practice leads to Master-ing the technique!
Unusual Muscles and EMG
Eric J. Sorenson, MD
DISCLOSURE Relevant Financial Relationship(s)
None
Off Label Usage
None
Learning Objectives
• Understand the indications to study uncommon muscles
• Localizing value of uncommon muscles • Risks associated with uncommon muscles
Reference
Anatomical Guide for the Electromyographer: The limbs and trunk
Third Edition, Thomas Books, Springfield, IL
Authored by: Aldo O. Perotto
Case #1
55 year old man in good health. Noticed hand weakness, numbness and pain after an assault.
On examination: weakness and atrophy of the APB and Opponens
Normal strength in FDI and adductor
digiti minimi Normal reflexes at Biceps, Triceps and
brachioradialis
Median sensory (antidromic)
Median Motor
Median F-wave
Needle examination summary
Which muscle next?
Needle examination of which of the following muscles would provide the most localizing value:
A) 1st Lumbrical B) Flexor pollicis longus C) Extensor Indices Proprius D) Extensor Carpi Radialis
Flexor Pollicis Longus
Indications: 1. Localization of median nerve and anterior
interosseous nerve lesions or C8-T1 rootlesions
2. Most frequently used when the APB isabnormal in a median neuropathy at thewrist to check a distal median innervatedmuscle above the wrist to exclude amedian nerve lesion in the forearm
Problems: 1. Proximity to the radial artery2. Deep muscle, sometimes difficult to
locate, may be painful
First/Second Lumbrical
Indications: 1. Median nerve lesions, particularly
those that involve the very distalmedian nerve.
Problems: 1. Proximity to the digital nerve and the
tendons of other muscles2. Incorrect activation3. If too deep the adductor pollicis will
be punctured4. These muscles are subject to some
variation in innervation
Extensor Indices Proprius
Indications: 1. Useful in C8 radiculopathies and radial nerve lesions, especially those involving the posterior interosseous nerve
Problems: 1. Small thin muscle near the extensor pollicis longus and other thumb muscles2. Painful if enter tendons inadvertently
Extensor Carpi Radialis
Indications: One of the last muscles innervated bythe radial nerve before it becomes theposterior interosseous nerve
Pronator Quadratus
Indications: 1. Localization of median and anterior interosseous nerve lesions and C8-T1 root lesionsProblems: 1. Thin, deep muscle - can only be localized by activation of the muscle2. Needle must be positioned to pass between the two bones that are close together
Traumatic Proximal Median Mononeuropathy
Case #2
57 year old man with the onset of thigh pain and weakness following inguinal hernia repair 2 months prior to presentation. MRI of the lumbar spine was normal.
Case #2
Examination: Weakness in the hip adductors Normal strength in the vastus, rectus
femoris, iliopsoas Reflexes normal at the knee No discrete sensory loss
Sural Sensory
Peroneal Motor
Tibial Motor
Needle examination summary
Which muscle next?
Needle examination of which of the following muscles would best localize the lesion:
A) Tensor Fascia Lata B) Rectus Femoris C) Gracilis D) Sartorius
Gracilis
Indications: 1. Obturator nerve lesions and L4 radiculopathiesProblems: 1. A small, flat muscle that may be difficult to find especially in the obese and deconditioned patient
Tensor Fascia Lata
Indications: 1. L5 root lesions. Involvement of this muscle in L5 root lesions may be more obvious than the gluteus medius2. It is often easier to obtain minimal activation of only a few units in the TFL than in other proximal L5 muscles.Problems: 1. May be difficult to locate in the very obese patient2. If too anterior the needle will enter the rectus femoris
or sartorius.
Rectus Femoris
Sartorius
Obturator neuropathy due to metastatic disease
Case #3
55 year old man with the spontaneous onset of severe pain over his scapula 1 year prior. This lasted a few days and gradually improved over a few weeks. As his pain improved he noticed weakness in his right shoulder which has persisted.
Examination
Strength: Normal with the exception of right scapular winging
Reflexes: Normal at Biceps, Triceps and
Brachioradialis Sensory: Normal
Needle examination summary
Which muscle?
Which of the following unusual muscles is most likely to be abnormal?
A) Serratus Anterior B) Levator Scapulae C) Teres Minor D) Latissimus dorsi
Serratus Anterior
Indications: 1. Winging of the scapula2. Unexplained shoulder pain3. Examining the most proximal branch of the C5, C6, and C7 spinal nerves after the posterior primary ramiProblems: 1. The risk of inadvertently entering the lung especially in obese and uncooperative patients
Trapezius
Indications: 1. Scapular winging2. Lesions of the lower cranial nerves or upper cervical spine3. Proximal muscle weakness4. Shoulder pain syndromes
Levator Scapulae
Indications: 1. Very proximal C4 and C5 muscle that may be more easily isolated than the rhomboids 2. The dorsal scapular nerve (C5) comes off the upper trunk just distal to the long thoracic nerve, also receives innervation
from the dorsal primary rami of the C4 root Problems: 1. If needle inserted too posterior: trapezius will be entered 2. Too anterior: the sternocleidomastoid 3. If too superior: the splenius capitis
Teres Minor
Indications: 1. Axillary nerve lesions2. Shoulder painProblems: 1. Entering the wrong muscles: - too caudally: the teres major - too medially: the infraspinatus - too rostrally: the deltoid - too far lateral: the triceps
Latissimus Dorsi
Indications: 1. The most proximal posterior cord muscle before the middle trunk2. A proximal C7 muscle3. Neurologic dysfunction after shoulder dislocation4. Unexplained shoulder painProblems: 1. Muscle hard to locate in the obese and deconditioned patient, proximity to the pleural space
Traumatic long thoracic neuropathy
Case #4
58 year old man with progressive weakness and atrophy of his forearm muscles for past 10 months.
No pain No sensory loss
Examination
Weakness of his Finger extensors and wrist extensors
No sensory loss Preserved reflexes, including triceps and
brachioradialis
Radial Motor Study
Radial Sensory
Needle examination summary
Which muscle next?
Which of the following unusual muscles would be most informative next?
A) Extensor digitorum communis B) Supinator C) Flexor Carpi Radialis D) Anconeus
Anconeus
Anconeus
Indications: 1. Proximal to distal localization of a radial nerve lesion
Problems: 1. A thin muscle that is sometimes difficult to palpate and separate from the extensor carpi ulnaris muscle
Supinator
Indications: 1. C5-C6 radiculopathies and radial nerve lesions2. Just proximal to most lesions of the posterior interosseous nerveProblems: 1. Deep muscle, can only be reached by passing through other muscles
Extensor Digitorum Communis
Indications: 1. Useful in distinguishing C6 from C7 radiculopathies and radial nerve lesions, especially those involving the posterior interosseous nerve Problems: 1. Variable innervation between C7 and C8
Flexor Carpi Radialis
Indications: 1. Could be used in a suspected proximal median neuropathy if pronator teres is normalProblems: 1. If needle to deep it will be in the finger flexors2. If too lateral will be in pronator teres3. Very rarely examined
Intra-op recordings
Multifocal motor neuropathy with conduction block
Case #5
• 22 year old fire-fighter with 6 year history of progressive shoulder weakness, right greater than left
• Found at by primary caregiver to have a CK fluctuating between 500-1000
Examination
Strength: Weakness of his multiple shoulder girdle muscles right >>left Mild bifacial weakness Reflexes: Normal Sensory: Normal
Spinal Accessory Right
Spinal Accessory Left
Needle examination summary
Which muscle?
Which of the following unusual muscles will likely be helpful?
A) Diaphragm B) Intercostal muscles C) Rectus Abdominis D) Pectoralis Major
Pectoralis Major
Indications: 1. The sternal head is a rare proximal C8-T1 muscle and the medial pectoral nerve separates the lower trunk from the medial cord of the brachial plexus2. Myopathies affecting the shoulder girdle musclesProblems: 1. Difficult to separate the two heads, multiple root innervation, proximity to pleural space
Diaphragm
Indications: Phrenic nerve lesions Respiratory insufficiency, particularly ventilator
dependent patients of undetermined cause Some myopathies and motor neuron diseases Problems: Proximity of the liver and spleen Risk of pneumothorax In complete phrenic nerve lesions localization by
activation of MUPs is not possible In very chronic lesions, the muscle may become very
thin and thin difficult to localize
Diaphragm with US
Diaphragm with US
Diaphragm with US
Intercostal Muscles
Indications: 1. Intercostal nerve lesions, thoracic radiculopathy, atypical chest pain2. Segmental localization of intraspinal lesions3. Respiratory failure of possible neuromuscular cause
Problems: 1. These muscles are rarely examined because of the potential for a pneumothorax2. If they are examined the patient should be advised of the potential risk3. You minimize the risk of pneumothorax if you do not advance the needle past the point where you encounter motor units
Rectus Abdominis
Indications: 1. Lower thoracic or upper lumbar radiculopathies, intercostal, ilioinguinal, or iliohypogastric nerve lesions2. Patients with atypical abdominal or inguinal pain3. May help in segmental localization of intraspinal
Lesions
Problems: 1. Thin sheet like muscles: you may pass through more quickly than you expect2. A long (70 mm) needle may be required to reach them in the obese patient3. Careful attention to technique will make the chance of peritoneal
FSH dystrophy
Case #6
• 69 year old female with 2 year history of dysarthria and dysphagia
• Progressive for about 6 months and now stable last 18 months.
• Not fatigable • No Diplopia
Exam
• Extra-ocular movements normal, no ptosis, no fatigability
• Normal facial sensation, normal mastication • Normal facial strength • Normal hearing
Exam
• Absent gag • No palatal movement with phonation • Normal SCM and Trapezius strength • Mildly weak tongue, no atrophy or
fasciculations
• Flaccid, hypernasal dysarthria
Facial CMAP
Spinal Accessory CMAP
Which muscles?
Of the following muscles which would be most likely to be helpful?
A) Orbicularis Oculi B) Frontalis C) Masseter D) Tongue
Orbicularis Oculi
Indications: 1. Facial nerve or brainstem lesions, Bell's
palsy, hemifacial spasm2. Guillain-Barre syndrome3. Facial myopathies4. Motor neuron disease5. Flaccid dysarthriaProblems: 1. The muscle is thin and sometimes hard to locate
Frontalis
Indications: 1. Similar to the orbicularis oculi but also used for single fiber studies of a facial muscleProblems: 1. May be painful2. Very thin muscle3. Easy bleeding and bruising4. Maintain pressure over the site for a short time
Masseter
Indications: 1. Lesions of the trigeminal nerve2. Lower motor neuron lesions of the brainstem3. Myasthenia gravisProblems: 1. Poor relaxation.2. Some myasthenia gravis patients may have such marked involvement that motor units are tiny and resemble fibrillation potentials3. The muscle is covered by the platysma (facial nerve) and superficial insertion may reveal the smaller MUPs of the platysma
Tongue
Indications: 1. Lesions of the hypoglossal nerve and twelth nerve nucleus2. motor neuron disease3. flaccid dysarthria4. myasthenia gravisProblems: 1. Relaxation often poor and difficult to see fibrillation potentials if they are infrequent2. Small size of normal motor unit potentials may allow misinterpretation as fibrillation potentials
Needle examination
Collette-Sicard Syndrome
EMG Waveform Analysis
Devon I. Rubin and Elliot L. Dimberg Mayo Clinic
Jacksonville FL
EMG Waveform Analysis Session
This Morning: #1 - Basics of EMG Waveform Recognition Review of spontaneous discharges #2 – Basics of MUP Analysis This Evening:
Rapid Quantitation of MUP Testing your skills with Case Examples and Quizzes Fun !
EMG Waveform Analysis Recording and analyzing the electrical activity of the muscle
fibers in motor units in the muscle
Unique combination of knowledge and skills
Basic Pattern Recognition • EMG: highly complex patterns
• Existing, automatic skill
• Recognition skill is instantaneous
– Simultaneous types and numbers
• Learn by: – Hearing > seeing – Naming – Comparison with others – Repetition
• Categorize waveform by pattern
Fibrillation potentials
Myotonic discharges
Complex repetitive discharge
Motor unit potential
End plate spikes
Myokymic discharges
EMG Potentials
End plate spike
Varying MUP
Long duration MUP
Characterization by Origin of EMG Potentials
Single Muscle Fibers
Firing Alone • End plate spikes • Fibrillation potentials • Myotonic discharges
Firing in Groups • Adjacent muscle fibers -
• Complex Repetitive Discharge • Insertion activity
• Motor unit potentials -Spontaneous • Fasciculation potentials • Myokymic discharges • Neurotonic discharges
• Motor unit potentials - Voluntary
Characterization by Signal Recognition
• Listen: – Firing pattern (Regular,
Irregular, Semi-rhythmic) – “Sounds like . . . .”
• Look:
– Configuration (Triphasic, biphasic, positive/negative)
Triphasic Muscle Action Potential
Nerve Terminal
=
+++ - - - - +++
+++ - - - - +++ +++ - - - - +++
+++ - - - - +++ +++ - - - - +++
EH Lambert
Firing Patterns of EMG Potentials
Semi-Rhythmic: (10% variation) (motor unit potential) I I I I I I I I I I I I I I I
Regular: linear change(1% variation) (fibrillation potential) I I I I I I I I I I I I
Regular: no change (complex repetitive discharge) I I I I I I I I I I I I I I I I I I I I I I I I I I I I I I
Regular: exponential change, wax/wane (myotonic) I I I I I I I I I I I I Irregular: (random change) (end plate spike) I I I I I I I I I I I I I I I
Bursts: (single or multiple MUP) – Regular or semi-rhythmic
Fibrillation Potentials
Action potentials of individual muscle fibers in the absence of innervation FIRING PATTERN: Regular 0.5 - 15 per second FORM: • Spikes - Biphasic or triphasic, 50-300 microvolts “tick-tick” • Positive waves - Biphasic, long rise time “tock-tock”
Fibrillation Potentials Spike form
Positive wave form
Regular: steady change (fibrillation potential) (0.5-15 Hz) I I I I I I I I I I I I
Fibrillation Potential
200
250
300
350
400
450
500
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22
Sequential Spikes
Inte
rspi
ke In
terv
al (m
s)
Potentials recorded from a single muscle fiber by two electrodes along the fiber
(The potentials are initiated by movement of electrode #1)
Electrode #1
Electrode #2
EH Lambert
Triphasic Fibrillation Potential
Site of generation of fibrillation potential
=
+++ - - - - +++
+++ - - - - +++ +++ - - - - +++
+++ - - - - +++ +++ - - - - +++
Positive wave Fibrillation Potential
=
+++ - - - - +++
+++ - - - - +++ +++ - - - - +++
+++ - - - - +++ +++ - - - - +++
Site of generation of fibrillation potential
1+ Persistent single trains
2+ - Moderate numbers
3+ - Many in all areas
4+ - Completely fill baseline
Grading Fibrillation Potentials
EH Lambert
Fibrillation Potentials Associated Disorders
Neurogenic • Anterior horn cell disorders – e.g. ALS • Radiculopathies – “active” • Mononeuropathies – “severe” • Axonal peripheral neuropathies
Myopathic • Inflammatory (e.g. polymyositis, IBM) • Toxic myopathies (e.g. statin myopathy) • Muscular dystrophies • Rhabdomyolysis
Severe NMJ disorders • Myasthenia gravis (severe) • LEMS • Botulism
• Fiber necrosis • Fiber splitting • Vacuolar damage
Fibrillation Potential Origin and Cessation in Myopathies
Muscle fiber necrosis
Vacuolar destruction
Muscle fiber splitting
Muscle fiber reinnervation
Endplate spikes and noise
Spike
Noise
Firing pattern: irregular, rapid Biphasic - initial negativity
Irregular (end plate spike) I I I I I I I I I I I I I I I
Miniature end plate potentials Firing pattern: irregular, rapid
0
50
100
150
200
250
300
350
1 11 21 31 41 51 61 71 81 91 101 111 121 131 141 151 161 171
Sequential Spikes
Inte
rspi
ke In
terv
al (m
s)
AT
Myotonic Discharges
Regular: exponential change, wax/wane (myotonic) I I I I I I I I I I I I
Spike
Positive waveform
Decreasing rate & amplitude
Increasing rate & amplitude
Myotonic Discharges Associated Disorders
Neurogenic • Axonal peripheral neuropathies – RARELY • Severe, old neurogenic disorders - RARELY
Myopathic - Prominent • Myotonic dystrophy**
– DM1 – DM2 (PROMM)
• Myotonia congenita** • Paramyotonia congenita** • Hyperkalemic periodic paralysis
Myopathic – Occasional • Polymyositis • Acid maltase deficiency • Drug - induced myotonia
– cholesterol lower agents, colchicine
** with clinical
myotonia
Complex Repetitive Discharges
• Fast or slow (3 – 40 Hz) • Configuration: (3-10 spikes, stable or unstable)
Regular: fixed intervals (abrupt onset, cessation, change) I I I I I I I I I I I I I I I I I I I I I I I I I I I I I I
Complex Repetitive Discharge Ephaptic transmission from neighboring muscle fibers
=
+ +
+ +
=
Complex Repetitive Discharges Associated Disorders
Neurogenic – CHRONIC DISORDERS • Anterior horn cell disorders – e.g. ALS, SMA • Radiculopathies – “chronic, old” • Axonal peripheral neuropathies - longstanding
Myopathic - CHRONIC • Inflammatory (e.g. IBM) • Muscular dystrophies
Normal • Iliopsoas • Biceps
Fasciculation Potentials
Origin - AHC, axon, nerve terminal FIRING PATTERN
•Single, random, irregular •1 - 100 per minute
FORM •No standard configuration •Resemble motor unit potentials •Often distant
Sound: “rain on a roof”
Fasciculation Potentials Associated Disorders
Neurogenic • Anterior horn cell disorders – e.g. ALS, SMA • Radiculopathies • Axonal peripheral neuropathies
Other • Hyperexciteable nerve syndromes (“cramp-fasciculation
syndrome”) • Tetany • Hyperthyroidism • Anti-cholinesterase medication (e.g. Mestinon)
Normal • Benign fasciculations
• Pearl: Long duration, polyphasic
(complex) fasciculation – more suggestive of a neurogenic disorder
Myokymic Discharges
• 1 or few MUP firing repetitively in bursts • Burst Pattern: Regular or Semi-rhythmic
Myokymic Discharges Associated Disorders
Extremities • Radiation • Chronic nerve compression (CTS) • AIDP, CIDP • Gold therapy • Rattlesnake venom
Facial • Multiple sclerosis Tuberculoma • Brainstem glioma Sarcoidosis • Polyradiculopathy Meningeal carcinomatosis • Facial palsy Syringobulbia • ALS
Neuromyotonic Discharges • Spontaneous MUP • Regular (wane) • Very high frequency (200-300 Hz)
– Continuous single MUP firing or – Discontinuous bursts
• “Indy (NASCAR) racecar”
Neuromyotonic Discharges Associated Disorders
• Voltage-gated, potassium channel disorders – “Continuous muscle fiber activity” – “Isaac’s syndrome”
• Anticholinesterase poisoning • Tetany • Chronic spinal muscular atrophies • Intra-operative nerve irritation
Voluntary Motor Unit Potential Gastrocnemius medialis
130 msec 140 msec 150 msec 135 msec 140 msec
Voluntary Motor Unit Potentials
• Configuration: Triphasic, initial positive (occasionally negative), 6-15 msec duration
• Sound: “ataxic clock”
Semi-Rhythmic (5-40 Hz) – Limited (10%) variation I I I I I I I I I I I I I I I
What is the best way to recognize motor unit potentials?
Semi-rhythmic firing pattern
Motor Unit Potential
0
50
100
150
200
250
300
350
400
1 4 7 10 13 16 19 22 25 28 31 34 37 40 43 46 49 52 55 58 61 64 67 70 73 76 79 82 85
Sequential Spikes
Inte
rspi
ke In
terv
al (m
s)
Motor Unit Potentials
A Single Motor Unit All the muscle fiber innervated by the AHC.
Motor Unit Recording Multiple A Single Muscle Fiber Action Potential
Motor Unit Recording Multiple (2-15) Muscle Fiber Action Potentials
Factors Affecting MUP Morphology
Technical – Electrode type
• Recording surface area
– Filter settings – Amplifier
characteristics
Physiologic – Muscle
– Subject’s age
– Temperature
G1
G1
G2
G1
G2
Concentric
Monopolar
Single Fiber
Pick Up Area
Pick Up Area
Technical Factors Needle Electrode Types
Effect of Needle Electrode Position Same Motor Unit, Different Muscle Fiber Locations
=
Distant
Near
Asynchrony
Shaft
Filters
Physiologic Factors Affecting MUP
• Low Temperature (or fiber diameter) – Slows muscle fiber action potential CV, increase temporal dispersion
– MORE COMPLEXITY – LONGER DURATION
– Increases muscle fiber action potential amplitude
• Age – MUP amplitude, duration, and turns increases with age (distal leg muscles)
• Muscle – Frontalis < Biceps < Anterior tibialis
MUP Parameter Determinants Muscle Configuration
Number of motor units - 50-600 motor units per muscle
Innervation ratio - 5-2000 muscle fibers per motor unit
Fiber density - 25-200 per square millimeter Motor unit area –
2-15 mm diameter
MUP Parameters Assessed • Rise time
– Distance from muscle fibers
• Spikes, turns, phases – Fiber number, synchrony
• Duration • Fiber size, density, synchrony
• Stability – NMJ and nerve terminal
• Recruitment • Number of motor units
Rise Time
Duration
Amplitude
Turns
Satellite
Temporal Course of EMG changes in acute neurogenic disorders
(severity dependent) 1 week 2 weeks 6 weeks 6 months
Fibrillation Potentials
None Some Many None (Tiny)
Recruitment Reduced Reduced Reduced Reduced
Phases Normal Polyphasic Polyphasic Normal (polyphasic)
Duration Normal (Long) Long Long
Other None Unstable Unstable CRD Fascics
Neurogenic Disorders MUP Changes
Loss of axons • Reduced number of
MUP • Reduced recruitment
Collateral sprouting • Loss of synchrony of
fibers • Change in appearance
X
Temporal Course of MUP Changes Acute Neurogenic Injury
Normal
Immediate Reduced Recruitment
1 months post Unstable MUP, turns
2-6 months Polyphasic, long duration
> 6 mo Long duration
MUP Parameters
• Rise time – Distance from muscle fibers
• Spikes, turns, phases • Fiber number, synchrony
• Duration • Fiber size, density, synchrony
• Stability • NMJ and nerve terminal
• Recruitment • Number of motor units
Rise Time
Duration
Amplitude
Turns
Satellite
Temporal Course of MUP Changes Acute Neurogenic Injury
Normal
Immediate Reduced Recruitment
1 months post Unstable MUP, turns
2-6 months Polyphasic, long duration
> 6 mo Long duration
MUP Recruitment MUP Firing Rate with Effort
MUP1 MUP2
MUP3
MUP4
Force
Mild Moderate Strong
MUP Firing Rate
0
5
10
15
20
25
50 ms
50 ms
50 ms
50 ms
50 ms
50 ms
Reduced Recruitment
Reduced Recruitment
MUP1
MUP2 MUP3
Force
Mild Moderate Strong
MUP Firing Rate
0
5
10
15
20
25
“Poor Activation”
MUP1 MUP2
Force
Mild (Strong)
MUP Firing Rate
0
5
10
15
20
25 Effort Pain Central Disorder Stroke Myelopathy
Rapid Recruitment Assessment is Effort-Dependent !
MUP1 MUP2
MUP3
MUP4
Force
Mild Moderate Strong
MUP Firing Rate
0
5
10
15
20
25
Recruitment frequency is normal Ratio of rate: number < 5 Multiple MUP with minimal effort (“all or none pattern”)
Recognizing Reduced Recruitment
• Compare ratio of rate: number with normal for that muscle
• Most limb muscles have ratio of rate:number of < 5
– 15 Hz: 3 MUP – 20 Hz: 4 MUP
• Learn more tonight
Disorders With Reduced Recruitment
*Hallmark of a neurogenic process* Proportional to loss of axons
Neurogenic • Axon destruction (e.g. nerve laceration, radiculopathies,
neuropathies) • Loss of anterior horn cells (e.g. ALS) • Conduction block (e.g. Saturday night palsy)
Myopathies • Severe myopathy with loss of all muscle fibers in some
motor units (e.g. end-stage muscular dystrophy)
Stages of Reinnervation Collateral Sprouting
a) UNSTABLE NMJ TRANSMISSION Decrement on repetitive stimulation Motor unit potential variation
b) ALTERED FIBER NUMBER AND SYNCHRONY MUP configuration change MUP size change
Recognizing MUP Changes Neurogenic Diseases
Normal
Immediate Reduced Recruitment
1 months post Unstable MUP
2-6 months Polyphasic
6 mo - 2 yrs Long duration
Motor Unit Potential Stability
Stable
Unstable (varying)
Motor Unit Potential Variation Blocking of Muscle Fibers
Disorders with Motor Unit Potential Variation
Neurogenic • Ongoing reinnervation after axonal loss
– e.g. ALS, recovering radiculopathy or mononeuropathy, reinnervating neuropathy
Myopathies • Reinnervating muscle fibers
NMJ disorders • Myasthenia gravis (severe) • LEMS • Botulism
Temporal Course of MUP Changes Acute Neurogenic Injury
Normal
Immediate Reduced Recruitment
1 months post Unstable MUP, turns
2-6 months Polyphasic, long duration
> 6 mo Long duration
Polyphasic MUP Neurogenic - Asynchronous Firing
=
+
+ +
=
+
Polyphasic MUP Myopathy
+ +
+
=
+
“Nascent” MUPs • Reinnervation after severe axon loss
– Atrophic muscle fibers – Temporally dispersed
• immature myelination • small muscle fibers
– Asynchronous summation of only few fibers – Unstable NMJ transmission
• Low amplitude, polyphasic, varying MUP – Short, normal, or long duration
& REDUCED RECRUITMENT
Recognizing MUP Changes Neurogenic Diseases
Normal
Immediate Reduced Recruitment
1-2 months post Unstable MUP
2-6 months Polyphasic
6 mo - 2 yrs Long duration
Normal Motor Unit Potential
“Neurogenic” Motor Unit Potential
Motor Unit Potential Changes in Myopathies
• Reduced motor unit territory – Reduction of # of muscles fibers / motor unit – Reduction in muscle fiber size
• Decreased duration of MUP • Decreased amplitude of MUP • Increased phases of MUP (desynchrony)
Normal Motor Unit Potential
“Myopathic” Motor Unit Potential
Disorders with Short Duration MUPs (not necessarily “myopathic”)
Neurogenic • Early reinnervation from severe nerve damage
(“nascent MUP”)
Myopathic • Inflammatory (e.g. polymyositis, IBM) • Toxic myopathies • Muscular dystrophies • Myotonic dystrophy • Congenital myopathies
NMJ disorders • Myasthenia gravis • LEMS • Botulism
EMG Waveform Analysis Session
This Evening: Practice assessment of recruitment and other
MUP parameters Testing your skills with Quizzes and Case
Examples
Questions and Answers this Evening
Crafting the EMG Report
Benn E. Smith, M.D. Department of Neurology
February 2015
Disclosure
Relevant Financial Relationship(s) None
Off Label Usage
None
What is all the fuss?
1) Why discuss this topic at all? 2) Isn’t it obvious how to write an EMG report? 3) Shouldn’t we be spending more time on learning the technical nuances of EMG? 4) Did we have trouble finding useful topics to fill the EMG course program?
Problems with EMG Reporting 1) The topic is not well covered in most training programs 2) We have difficulty summarizing EMG/NCS data 3) We are preoccupied by the electrical 4) We neglect the non-electrical clinical 5) We have problems writing clearly and accurately 6) It is easier not to take responsibility in writing an EMG report
Craft (\ 'kraft \) vt: to make or produce with care, skill, or ingenuity (a carefully ~ed story)
What do we mean by “craft”?
There is a hole in our training
1) EMG reports have a reputation of being difficult to understanding and of marginal clinical utility 2) Even though a physician may be a masterful electromyographer, she may have not done so well in English composition 3) There is so much to learn on the technical side of doing EMG/NCS, skills in putting together an excellent report are sometimes neglected
Our difficulty summarizing electrophysiologic data
1) There is a widespread tendency to repeat all data in the interpretation (and present little -- if any -- synthesis) 2) EMGers often are meticulous about identifying every “tree,” while doing poorly at succinctly describing the affected “glen” or “forest”
Our difficulty summarizing electrophysiologic data
3) EMGers often focus too narrowly on the details of electrophysiologic values and miss “the elephant in the room,” that is, the historical clues and physical findings that clearly point to an alternative diagnosis
EMG #1 referral indication: “paresthesia and pain” Summary: The left median antidromic sensory response amplitude was 10 µV (nl > 15 µV) with a conduction velocity of 53 m/s (nl > 54 m/s) and a distal latency of 4.5 ms (nl < 3.6 ms). The left ulnar antidromic sensory response was 5 µV in amplitude (nl > 10 µV) with a conduction velocity of 51 m/s (nl > 53 m/s) and a distal latency of 3.3 ms (nl < 3.2 ms). The left median/APB motor amplitude was the 4.2 mV (nl > 4 mV) with conduction velocity of 49 m/s (nl > 48 m/s) and a motor distal latency of 5.2 msec and an F wave latency of 30 ms (nl < 32 ms). The left ulnar/ADM motor amplitude was 6.1 mV (nl > 6 mV) with a conduction velocity of 47 m/s (nl > 51 m/s) and a motor distal latency of 3.4 ms (nl < 3.6 ms) and an F wave latency of 29.7 ms (nl < 33 ms). The left fibular/EDB motor response was 1.0 mV in amplitude (nl > 2.0 mV) with a conduction velocity of 38 m/s (nl > 41 m/s), a motor distal latency of 5.0 ms (nl < 6.6 ms) and no elicitable F waves. The left sural sensory response was 2.2 µV in amplitude (nl > 6 µV) with a distal latency of 4.6 ms (nl < 4.5 ms). Concentric needle examination showed large motor unit potentials in the left first dorsal interosseous, abductor pollicis brevis, tibialis anterior, and medial gastrocnemius muscles with fibrillation potentials in the abductor hallucis muscles on both sides and a single train of positive sharp waves in the left low lumbar paraspinal muscles.
Interpretation: The EMG findings suggest either median, ulnar, fibular, and tibial mononeuropathies (multiple mononeuropathies), polyneuropathy with superimposed carpal tunnel syndrome, polyradiculoneuropathy, or motor neuron disease with an additional sensory neuropathy. Multilevel cervical and lumbosacral radiculopathy or plexopathy cannot be completely excluded. Suggest clinical correlation.
Report Assessment?
The cluttered noncommittal report
Comment: Regurgitation of detailed individual data elements with no useful summary or pattern recognition. Noncommittal interpretation with no attempt at correlating the findings with the patient’s symptoms and signs.
EMG #2 referral indication: “paresthesia and pain” Summary: NCS showed low amplitude sensory and motor responses with borderline NCVs and disproportionate prolongation of the left median sensory and motor distal latencies. Concentric needle examination demonstrated mild distal MUP enlargement accompanied by low-grade irritability and fibrillation potentials limited to intrinsic foot muscles. The patient reported no hand symptoms whatsoever. Tinel sign was absent over the median nerves at the wrists. Mild left thenar atrophy noted of which the patient was unaware.
Interpretation: The EMG findings suggest electrophysiologically mild to moderate predominantly axonal sensorimotor peripheral neuropathy with superimposed asymptomatic left median neuropathy at the wrist.
Report Assessment?
The tailored “nickel on the table” report
Comment: Summarized individual data elements with findings presented in a cohesive clinically pertinent pattern. Interpretation commits to a particular diagnostic formulation (polyneuropathy and subclinical median neuropathy at the wrist) correlating the findings with the patient’s symptoms and signs.
Our preoccupation with the electrical
1) We reduce impedance, attach wires, turn dials, and administer current pulses 2) We collect waveforms, analyze responses, move cursors, record detailed numbers 3) We report nerve conduction values to 2 decimal places, list muscles with long Latin names, describe MUP morphology, and obsess over charts with myriad pluses and minuses
Our neglect of the non-electrical clinical
1) Time is short, patients are many, face-to-face physician-patient interactions are
brief 2) We rarely take the time to review key elements of the presenting complaints, the pace of development of symptoms, or exacerbating and ameliorating factors 3) We tend to rely heavily on the referral indications and the history taken by the referring physician
“Typical” EMG Referral Indications 1) Pain
Dysparenuia
Charcot joint, check anal EMG
Pain in the neck
2) Sensory EMG for worms crawling in leg
Thing numbness
3) Incomplete understanding of EMG lower limb numbness, r/o CTS r/o lower extremities carpool tunnel reptile dysfunction 4) ????? EMG for mental stenosis my apathy patient leaving town
“Typical” EMG Referral Indications
EMG #3 referral indication: “unsteadiness” Summary: NCS and concentric needle examination of the lower limbs were normal.
Interpretation: Normal EMG. This study provides no evidence for peripheral neuropathy or any other neuromuscular explanation for the patient’s unsteadiness.
Report Assessment?
Failure to Make Pertinent Clinical Observations during EMG Testing
Comment: Focus is purely on the electrophysiology, ignoring obvious clinical signs and symptoms at the time of the examination (see below)
EMG #4 referral indication: “unsteadiness” Summary: NCS and concentric needle examination of the lower limbs were normal. Every needle insertion below the knee on either side resulted in either an extensor plantar response or triple flexion. Physical examination showed no upper limb deep tendon reflexes, markedly hyperactive lower limb reflexes, sustained bilateral ankle clonus, and bilateral extensor plantar responses. No sensory level to pin prick could be demonstrated on the torso either anteriorly or posteriorly. Interpretation: Normal EMG. Although this study does not suggest a peripheral process, the physical findings described above are those of a bilateral central nervous system disorder affecting upper motor neuron pathways. Neurologic consultation is recommended. Results discussed by telephone with Dr. Jones.
Report Assessment?
Pertinent Clinical Observations during EMG Testing Help the Referring Clinician
Comment: while electrophysiological findings are presented, the emphasis is put on clinical observations which re-direct the neurologic evaluation
4) Patients often “change their tune” between the initial H and P and their EMG visit 5) Patients often use medical terms (“paresthesia”, “sciatica”, etc.) during their initial H and P which have not been explored further by the referring physician 6) Limb pain is often equated with a neurogenic etiology, leading to low yield referrals for “radicular” or “neurogenic” pain
Our neglect of the non-electrical clinical
EMG #5 referral indication: “Right hip/leg pain”
Summary: NCS showed a low amplitude right fibular /EDB compound muscle action potential and absent right fibular/EDB F waves. Concentric needle examination demonstrated large motor unit potentials in the right L5 territory both distally and proximally, unaccompanied by irritability or fibrillation potentials in the leg, hip girdle, or lumbar paraspinal muscles. Interpretation: The EMG findings are those of right L5 radiculopathy.
Report Assessment?
Failure to Discount the EMG Findings as Being Clinically Insignificant
Comment: although the EMG and NCS findings are correctly described and interpreted, the electromyographer does not “go to the next level” and weave them into the prior clinical history, taking into account other possible explanations for the current symptoms.
EMG #6 referral indication: “Right hip/leg pain” Summary: NCS showed a low amplitude right fibular /EDB compound muscle action potential and absent right fibular/EDB F waves. Concentric needle examination demonstrated large motor unit potentials in the right L5 territory both distally and proximally, unaccompanied by irritability or fibrillation potentials in the leg, hip girdle, or lumbar paraspinal muscles. The patient reported having an episode of severe low back and radiating right lower limb pain twelve years ago associated with a transient right foot drop. The problem resolved spontaneously over 3-4 months. Physical examination currently shows normal lower extremity strength and marked pain on flexion, abduction, and external rotation of the right hip. Interpretation: Although the EMG findings provide evidence of electrophysiologically old inactive right L5 radiculopathy, the current symptoms are perhaps more likely to be due to mechanical disease of the right hip joint.
Report Assessment?
This Report Looks Beyond the “Tree” to see the Forest
Comment: the same NCS and EMG observations are made, but this time with the added depth of relevant past medical history and current physical examination abnormalities which lead to the correct diagnosis.
Our problem taking responsibility 1) The EMG report often presents findings in isolation without an attempt to comment on clinical relevance 2) The EMG report which recommends “clinical correlation” gives the impression that the EMGer is somehow absolved of integrating the EMG results into the clinical context 3) The EMG report should not only rely on electro- physiologic findings, but instead should incorporate all clinically relevant data available to the EMGer
1) The referring physician is looking for help in coming up with a valid explanation for the patient’s symptoms
Conclusions
2) Try to develop a “big picture” approach to framing results of the EMG (“tell the story”)
• leave minutia in the data section • “What would I want from the report if
this were my patient?” • don’t be afraid of expressing
uncertainty or doubt in the report
Conclusions
3) Performing a brief history and physical examination is time well spent in the EMG Laboratory – we are physicians
Conclusions
Craft (\ 'kraft \) n: an occupation or trade requiring manual (or mental) dexterity or artistic skill (the sculptor’s ~)
Craft is also a Noun
EMG Waveform Analysis
Evening Workshop
Evening Workshop Outline
#1 – Unknown quiz
#2 – Learn Rapid Auditory Quantitation of MUP parameters
#3 – “Who Wants to be an Electromyographer?”
#4 - Bedtime (or breakfast)
EMG Waveform Analysis – Skills to Master• Pattern Recognition• Semi-quantitation
Analysis of Motor Unit Potentials 42 year old with arm pain - Needle EMG of Deltoid
How do you know?Is this potential normal or abnormal?
How much time (on average) do you spend analyzing MUP in a muscle?
1. >10 minutes2. 5 – 9 minutes3. 1 – 4 minutes4. < 1 minute
Motor Unit Potential ConfigurationRecording Multiple (2-15) Muscle Fiber Action Potentials
Quantitation In Electrodiagnosis
NCS
• Voluntary needle EMG activity• Limited use in USA• More common in Europe• New programs
Repetitive stimulation
MUP Quantitation - Single MUP methodEffective but still time consuming
MAYO MUP ABNORMALITY GRADING BY MEAN VALUE IN MSEC AT AGE 20Lower and upper limit of normal (from Buchthal 1955)
0 ± + ++ +++ ++++
1st dorsal interos. 8.0, 12.2 7.0,13.1 6.0,14.1 5.0,15.0 4.0, 16.0 <4.0, >16.0
Deltoid 8.2,12.2 7.1,13.3 6.1,14.3 5.1,15.3 4.1,16.3 <4.1, >16.3
Triceps 9.3,13.9 8.1,15.1 7.0,16.2 5.8,17.4 4.6,18.6 <4.6, >18.6
Biceps 8.0,12.0 7.0,13.0 6.0,14.0 5.0,15.0 4.0,16.0 <4.0, >16.0
Anterior tibial 9.8,14.8 8.6,16.0 7.4,17.2 6.2,18.5 4.9,19.7 <4.9, >19.7
Vastus medialis 8.2,12.2 7.1,13.3 6.1,14.3 5.1,15.3 4.1,16.3 <4.1, >16.3
Medial gastroc. 7.5,11.3 6.6,12.2 5.6,13.2 4.7,14.1 3.8,15.0 <3.8, >15.0
Opponens pollicis 7.3,10.9 6.4,11.8 5.5,12.7 4.6,13.7 3.6,14.6 <3.6, >14.6
Peroneus longus 7.8,11.8 6.9,12.7 5.9,13.7 4.9,14.7 3.9,15.7 <3.9, >15.7
Gluteus maximus 9.6,14.4 8.4,15.6 7.2,16.8 6.0,18.0 4.8,19.2 <4.8, >19.2
Low cervical psp. 8.6,12.8 7.5,13.9 6.4,15.0 5.4,16.1 4.3,17.1 <4.3, >17.1
Automated MUP AnalysisComputer does all the work
• Averaged MUP quantitation (AMUP)
•McGill & Dorfman 1989• Multiple MUP
quantitation (MMUP)•Stalberg 1995
• Decomposition EMG (DQEMG)
•Stashuk & Doherty 2003
• Rapid MUP quantitation
•Lambert - back to the future
What is “Rapid Quantitation”?
Obtain a numerical value
without measurement
Estimate Your Pulse Rate(Per minute)
1. Under 562. 56 – 603. 61 – 654. 66 – 705. 71 – 756. 76 – 807. 81 – 858. 86 – 909. Over 90
Let’s Learn Rapid Quantitation
1. Identify the waveform by pattern recognition
2. Learn rapid quantitation (train your ears)
3. Test your rapid quantitation
Let’s Learn Rapid Quantitation
1. Identify the waveform by pattern recognition
2. Learn rapid quantitation (train your ears)
3. Test your rapid quantitation
MUP Parameters to Learn
• Rise timeDistance from muscle fibers
• RecruitmentNumber of motor units
• StabilityNMJ and nerve terminal
• Spikes, turns, phasesFiber number, synchrony
• DurationFiber size, density,
synchrony
Rise Time
Duration
Amplitude
Turns
Satellite
How Close is the Potential?Your ear will tell you!
Based on slew rate/rise time
Your ear hears the slew rate = rate of rise (mV/msec)
Rise time = time (msec) from peak positivity to peak negativity
Rise time depends on slew rateand amplitude
=
Rise time
Slew rate
=
Rise time
Slew rate
Practice Rise Time with EMG Simulator
MUP Changes to Quantitate in Neurogenic Diseases
Normal
ImmediateReduced Recruitment
1 monthsUnstable MUP
2-6 monthsPhases
6 mo - 2 yrsDuration increase
50 ms
50 ms
50 ms
Normal Recruitment
Orderly addition of potentials from different motor units with increase in discharge rate
MUP RecruitmentMUP Firing Rate with Effort
MUP1MUP2
MUP3
MUP4
Force
Mild Moderate Strong
MUP Firing Rate(Hz)
0
5
10
15
20
25
MUP Recruitment
Number of motor units activeTwo sites - solid & dashed line
% of maximal contraction
Firing rate of multiple MUPat the two sites
Transient firing rate decrease with recruitment
From McGill Jour NS Methods 2005
50 ms
50 ms
50 ms
Reduced Recruitment
Too few MUP for rate of firing
Reduced Recruitment
MUP1
MUP2MUP3
Force
Mild Moderate Strong
MUP Firing Rate(Hz)
0
5
10
15
20
25
“Poor Activation”
MUP1MUP2
Force
Mild (Strong)
MUP Firing Rate(Hz)
0
5
10
15
20
25Effort PainCentral Disorder
StrokeMyelopathy
Recognizing Reduced RecruitmentEMG Simulator Exercise
• Step 1 - What is the firing rate of any individual MUP?• Step 2 - How many different MUP?• Step 3 - What is the ratio of rate to number?
• Compare ratio of rate: number (most limb muscles < 5)
• 15 Hz: 3 MUP, 20 Hz: 4 MUP
• Grading based on rate of firing of 1st MUP when 2nd MUP recruited:
1+ for >10 Hz2+ for >15 Hz3+ for > 20 Hz
Methods to Confirm Firing Rate1. Rate counter2. 50 msec/div – 20 div sweep – count the
number of MUP in 1 sec3. 10 msec/div sweep – count the interspike
interval and divide into 1000 msecINTERVAL (msec) FREQUENCY, Hz.
150 6.5125 8.0100 10.075 13.360 16.650 20.0
Firing Rate Confirmation
1 2 3 4 5 6 7 8 9
Recognizing Reduced RecruitmentEMG Simulator Exercise
• Step 1 - What is the firing rate of any individual MUP?• Step 2 - How many different MUP?• Step 3 - What is the ratio of rate to number?
• Compare ratio of rate: number (most limb muscles < 5)
• 15 Hz: 3 MUP, 20 Hz: 4 MUP
• Grading based on rate of firing of 1st MUP when 2nd MUP recruited:
1+ for >10 Hz2+ for >15 Hz3+ for > 20 Hz
MUP Parameters to Learn
• Rise time•Distance from muscle fibers
• Recruitment• Number of motor units
• Stability•NMJ and nerve terminal
• Spikes, turns, phases•Fiber number, synchrony
• Duration• Fiber size, density, synchrony
Rise Time
Duration
Amplitude
Turns
Satellite
Recognizing MUP ChangesEarly Reinnervation
Normal
ImmediateReduced Recruitment
1 months postUnstable MUP
2-6 monthsPolyphasic
6 mo - 2 yrsLong duration
Motor Unit Potential VariationBlocking of Muscle Fibers
MUP VariationBlocking of muscle fibers MUP Parameters to Learn
• Rise time•Distance from muscle fibers
• Recruitment• Number of motor units
• Stability•NMJ and nerve terminal
• Spikes, turns, phases•Fiber number, synchrony
• Duration• Fiber size, density, synchrony
Rise Time
Duration
Amplitude
Turns
Satellite
Recognizing MUP ChangesRemodeling
Normal
ImmediateReduced Recruitment
1 monthsUnstable MUP
2-6 monthsPolyphasic
6 mo - 2 yrsLong duration
MUP Parameters to Learn
• Rise time•Distance from muscle fibers
• Recruitment• Number of motor units
• Stability•NMJ and nerve terminal
• Spikes, turns, phases•Fiber number, synchrony
• Duration• Fiber size, density, synchrony
Rise Time
Duration
Amplitude
Turns
Satellite
Motor Unit “Remodeling”
Normal
Immediate
1 months post
2-6 months
6 mo - 2 yrs
ESS
Normal MUP
Long Duration MUPIncreased # fibers, fiber density
Disorders with Short Duration MUPs
• Myopathies
• Myasthenia gravis / LEMS• Early reinnervation after nerve
damage (nascent MUP)• Late stage neurogenic atrophy• Periodic paralysis
Normal MUP Short Duration MUP (Myopathy)